Fate and distribution of orally-ingested CeO2-nanoparticles based on a mouse model: Implication for human health

Abstract

The use of nanoparticles in agrichemical formula and food products as additives has increased their chances of accumulation in humans via oral intake. Due to their potential toxicity, it is critical to understand their fate and distribution following oral intake. Cerium oxide nanoparticle (CeO₂NP) is commonly used in agriculture and is highly stable in the environment. As such, it has been used as a model chemical to investigate nanoparticle's distribution and clearance. Based on their estimated human exposure levels, 0.15–0.75 ​mg/kg body weight/day of CeO₂NPs with different sizes and surface charges (30–50 ​nm with negative charge and <25 ​nm with positive charge) were gavaged into C57BL/6 female mice daily. After 10-d, 50% of mice in each treatment were terminated, with the remaining being gavaged with 0.2 ​mL of deionized water daily for 7-d. Mouse organ tissues, blood, feces, and urine were collected at termination. At the tested levels, CeO₂NPs displayed minimal overt toxicity to the mice, with their accumulation in various organs being negligible. Fecal discharge as the predominant clearance pathway took less than 7-d regardless of charges. Single particle inductively coupled plasma mass spectrometry analysis demonstrated minimal aggregation of CeO₂NPs in the gastrointestinal tract. These findings suggest that nanoparticle additives >25 ​nm are unlikely to accumulate in mouse organ after oral intake, indicating limited impacts on human health.